首页> 美国卫生研究院文献>Immunology >T-helper type-1-dominated lymph node responses induced in C57BL/6 mice by optimally irradiated cercariae of Schistosoma mansoni are down-regulated after challenge infection.
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T-helper type-1-dominated lymph node responses induced in C57BL/6 mice by optimally irradiated cercariae of Schistosoma mansoni are down-regulated after challenge infection.

机译:曼氏血吸虫最佳辐照尾optimal在C57BL / 6小鼠中诱导的T辅助1型占主导的淋巴结反应在感染后被下调。

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摘要

Following a single percutaneous vaccination with optimally irradiated cercariae of Schistosoma mansoni, C57BL/6 mice mount a T-helper type-1 (Th1) lymphocyte-dominant immune response and are highly resistant to challenge infection. In this study, we show that, besides interferon-gamma (IFN-gamma), lymph node (LN) cells draining the site of vaccination produce significant amounts of interleukin (IL)-4 and IL-10 in culture with parasite antigen. After a challenge infection at the original site of vaccination, these LN cells did not generate an anamnestic Th1 response. Paradosically, IFN-gamma production and cell proliferation were profoundly down-regulated, whereas IL-4 production was enhanced and occurred earlier than in challenge control cultures. When challenge was applied to a site remote from vaccination, IFN-gamma down-regulation was less evident, but the IL-4 response was consistently enhanced. Neutralization of IL-10 in vitro restored IFN-gamma production by LN cells, whilst IL-4 levels were reduced. These data indicate that down-regulation of IFN-gamma is controlled by IL-10 and/or IL-4. Mice showing down-regulated Th1 responses in the LN after S. mansoni challenge infection did not have a reduced ability to eliminate challenge parasites, indicating that the post-vaccination Th1 response had already armed the lungs with effector T cells before administration of challenge parasites. The observed phenomena of down-regulated Th1 and enhanced Th2 responses may be of relevance to other systems involving multiple infections or vaccination/boosting. Repeated applications to percutaneous sites having common lymphatic drainage would be expected to favour Th2 responses. Alternatively, in order to induce Th1-dominant responses and avoid unwanted IL-4/IL-10 induction, the use of remote sites is indicated.
机译:在对曼氏血吸虫进行最佳辐照尾的单次经皮疫苗接种后,C57BL / 6小鼠进行了以T辅助1型(Th1)淋巴细胞为主的免疫反应,并对攻击感染具有高度抵抗力。在这项研究中,我们表明,除干扰素-γ(IFN-γ)外,引流接种部位的淋巴结(LN)细胞在含有寄生虫抗原的培养物中还产生大量白介素(IL)-4和IL-10。在原始疫苗接种部位进行攻击感染后,这些LN细胞未产生记忆性Th1反应。荒谬的是,IFN-γ的产生和细胞增殖被大大地下调,而IL-4的产生则比攻击对照培养物中的产生要早。当将挑战应用于远离疫苗接种的部位时,IFN-γ的下调不太明显,但IL-4反应一直得到增强。 IL-10的体外中和恢复了LN细胞的IFN-γ产生,而IL-4的水平降低了。这些数据表明,IFN-γ的下调受IL-10和/或IL-4的控制。在曼氏沙门氏菌挑战感染后LN中显示Th1反应下调的小鼠消除攻击寄生虫的能力并未降低,这表明接种疫苗后Th1反应已经在给予攻击寄生虫之前用效应T细胞武装了肺。观察到的Th1反应下调和Th2反应增强的现象可能与涉及多重感染或疫苗接种/加强免疫的其他系统有关。预期重复施用于具有常见淋巴引流的经皮部位有利于Th2反应。备选地,为了诱导Th1占优势的反应并避免不期望的IL-4 / IL-10诱导,指示了使用远程位点。

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